Journal of Clinical Oncology, Vol 15, 1916-1922, Copyright © 1997 by American Society of Clinical Oncology
bcl-2, p53, and response to tamoxifen in estrogen receptor-positive metastatic breast cancer: a Southwest Oncology Group study
RM Elledge, S Green, L Howes, GM Clark, M Berardo, DC Allred, R Pugh, D Ciocca, P Ravdin, J O'Sullivan, S Rivkin, S Martino and CK Osborne
University of Texas Health Science Center at San Antonio, USA.
PURPOSE: To test the hypothesis that high bcl-2 expression and accumulation
of p53 protein, both of which should inhibit apoptosis, are associated with
a poorer tamoxifen response and a more aggressive clinical course in
estrogen receptor (ER)-positive metastatic breast cancer. METHODS: A total
of 205 paraffin-embedded tumor blocks were evaluated for nuclear p53 (a
marker of p53 inactivation) and cytoplasmic bcl-2 by immunohistochemistry
(IHC). All patients received tamoxifen as initial therapy for metastatic
disease. The study began in 1982 and follow-up duration of the 24 patients
last known alive is 8 years. RESULTS: Response to tamoxifen and time to
treatment failure (TTF) were not significantly associated with p53 status,
although patients with higher p53 had a worse survival (P = .008; median,
36 v 20 months). Higher bcl-2 expression was associated with higher levels
of ER (P = .02), better response to tamoxifen (62% v 49%; P = .07), longer
TTF (median, 9 v 5 months; P = .002), and better survival (median, 40
months v 25 months; P = .009). In multivariate analyses, including ER,
progesterone receptor (PgR), and p53, high bcl-2 remained significantly
associated with a longer TTF (P = .007) and survival (P = .07). p53 status
was a significant factor for shorter survival (P = .05), but not for TTF (P
= .61). CONCLUSION: p53 status, as determined by IHC is not significantly
associated with response to tamoxifen, although tumors with altered p53
protein are inherently more aggressive. Contrary to expectation, high bcl-2
identifies a relatively indolent phenotype of ER-positive metastatic breast
cancer, in which patients experience a better clinical response to
tamoxifen and a longer survival.
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